In silico design of a novel hybrid epitope-based antigen harboring highly exposed immunogenic peptides of BamA, OmpA, and Omp34 against Acinetobacter baumannii

鲍曼不动杆菌 生物信息学 巴马 表位 生物 微生物学 抗原 不动杆菌 病毒学 计算生物学 细菌 大肠杆菌 基因 免疫学 细菌外膜 抗生素 遗传学 铜绿假单胞菌
作者
Anahita Hessami,Zahra Mogharari,Fatemeh Rahim,Bahman Khalesi,Othman Jamal Nassrullah,Mohammad Reza Rahbar,Saeed Khalili,Abolfazl Jahangiri
出处
期刊:International Immunopharmacology [Elsevier BV]
卷期号:142 (Pt A): 113066-113066 被引量:6
标识
DOI:10.1016/j.intimp.2024.113066
摘要

Acinetobacter baumannii, is among the highest priority bacteria according to the WHO categorization which necessitate the exploration of alternative strategies such as vaccination. OmpA, BamA, and Omp34 are assigned as appropriate antigens to serve in vaccine development against this pathogen. Experimentally validated exposed epitopes of OmpA and Omp34 along with selected exposed epitopes predicted by an integrative in silico approach were represented by the barrel domain of BamA as a scaffold. Among the 8 external loops of BamA, 5 loops were replaced with selected loops of OmpA and Omp34. The designed antigen was analyzed regarding the physicochemical properties, antigenicity, epitope retrieval, topology, structure, and safety. BamA is a two-domain OMP with a 16-stranded barrel in which L4, L6, and L7 were the longest loops of BamA in order. The designed antigen consisted of 478 amino acids with antigen probability of 0.7793. The novel antigen was a 16-stranded barrel. No identical 8-meric peptides were found in the human proteome against the designed antigen sequence. The designed construct was safe regarding the allergenicity, toxicity, and human proteome reactivity. The designed antigen could develop higher protection against A. baumannii in comparison to either OmpA, BamA, or Omp34 alone.
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